Quantitative single-cell proteomics as a tool to characterize cellular hierarchies

Erwin M. Schoof(University of Copenhagen), Benjamin Furtwängler(University of Copenhagen), Nil Üresin(University of Copenhagen), Nicolas Rapin(University of Copenhagen), Simonas Savickas(Technical University of Denmark), Coline Gentil(University of Copenhagen), Eric R. Lechman(University Health Network), Ulrich auf dem Keller(Technical University of Denmark), John E. Dick(University Health Network), Bo Porse(University of Copenhagen)
Nature Communications
June 7, 2021
Cited by 346Open Access
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Abstract

Large-scale single-cell analyses are of fundamental importance in order to capture biological heterogeneity within complex cell systems, but have largely been limited to RNA-based technologies. Here we present a comprehensive benchmarked experimental and computational workflow, which establishes global single-cell mass spectrometry-based proteomics as a tool for large-scale single-cell analyses. By exploiting a primary leukemia model system, we demonstrate both through pre-enrichment of cell populations and through a non-enriched unbiased approach that our workflow enables the exploration of cellular heterogeneity within this aberrant developmental hierarchy. Our approach is capable of consistently quantifying ~1000 proteins per cell across thousands of individual cells using limited instrument time. Furthermore, we develop a computational workflow (SCeptre) that effectively normalizes the data, integrates available FACS data and facilitates downstream analysis. The approach presented here lays a foundation for implementing global single-cell proteomics studies across the world.


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